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Tetrabromobisphenol A Is an Efficient Stabilizer of the Transthyretin Tetramer

机译:四溴双酚A是运甲状腺素蛋白四聚体的有效稳定剂

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摘要

Amyloid formation of the human plasma protein transthyretin (TTR) is associated with several human disorders, including familial amyloidotic polyneuropathy (FAP) and senile systemic amyloidosis. Dissociation of TTR’s native tetrameric assembly is the rate-limiting step in the conversion into amyloid, and this feature presents an avenue for intervention because binding of an appropriate ligand to the thyroxin hormone binding sites of TTR stabilizes the native tetrameric assembly and impairs conversion into amyloid. The desired features for an effective TTR stabilizer include high affinity for TTR, high selectivity in the presence of other proteins, no adverse side effects at the effective concentrations, and a long half-life in the body. In this study we show that the commonly used flame retardant tetrabromobisphenol A (TBBPA) efficiently stabilizes the tetrameric structure of TTR. The X-ray crystal structure shows TBBPA binding in the thyroxine binding pocket with bromines occupying two of the three halogen binding sites. Interestingly, TBBPA binds TTR with an extremely high selectivity in human plasma, and the effect is equal to the recently approved drug tafamidis and better than diflunisal, both of which have shown therapeutic effects against FAP. TBBPA consequently present an interesting scaffold for drug design. Its absorption, metabolism, and potential side-effects are discussed.
机译:人血浆蛋白运甲状腺素蛋白(TTR)的淀粉样蛋白形成与多种人类疾病相关,包括家族性淀粉样变性多发性神经病(FAP)和老年性系统性淀粉样变性病。 TTR天然四聚体装配的解离是转化为淀粉样蛋白的限速步骤,该功能为干预提供了途径,因为适当的配体与TTR的甲状腺素激素结合位点的结合稳定了天然四聚体装配,并损害了转化为淀粉样蛋白的能力。 。有效的TTR稳定剂的期望特征包括对TTR的高亲和力,在其他蛋白质存在下的高选择性,在有效浓度下没有不利的副作用以及在体内的长半衰期。在这项研究中,我们表明常用的阻燃剂四溴双酚A(TBBPA)有效地稳定了TTR的四聚体结构。 X射线晶体结构显示TBBPA在甲状腺素结合袋中结合,其中溴占据三个卤素结合位点中的两个。有趣的是,TBBPA在人血浆中以极高的选择性结合TTR,其作用与最近批准的药物他法米地相当,且优于二氟尼沙胺,两者均显示出对FAP的治疗作用。因此,TBBPA提出了一种有趣的药物设计支架。讨论了其吸收,代谢和潜在的副作用。

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